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Publication : Development of Murine Systemic Lupus Erythematosus in the Absence of BAFF.

First Author  Stohl W Year  2020
Journal  Arthritis Rheumatol Volume  72
Issue  2 Pages  292-302
PubMed ID  31493335 Mgi Jnum  J:304900
Mgi Id  MGI:6510210 Doi  10.1002/art.41097
Citation  Stohl W, et al. (2020) Development of Murine Systemic Lupus Erythematosus in the Absence of BAFF. Arthritis Rheumatol 72(2):292-302
abstractText  OBJECTIVE: To determine whether systemic lupus erythematosus (SLE) can develop in the absence of BAFF in an SLE-prone host. METHODS: Starting with C57BL/6 mice that express a human BCL2 transgene (Tg) in their B cells (thereby rendering B cell survival largely independent of BAFF-triggered signals), we introgressed this Tg into NZM 2328 mice genetically deficient in BAFF (NZM.Baff(-/-) ) to generate NZM.Baff(-/-) .Bcl2(Tg) mice. Expression of human Bcl-2 and lymphocyte profiles were assessed by fluorescence-activated cell sorting, and serologic profiles were determined by enzyme-linked immunosorbent assay. Immunofluorescence and histologic analyses were performed to assess renal immunopathologic features in the mice, and clinical disease was assessed according to the outcomes of severe proteinuria and death. RESULTS: In comparison to their non-Tg NZM.Baff(-/-) littermates (n >/= 7), NZM.Baff(-/-) .Bcl2(Tg) mice (n >/= 8) overexpressed Bcl-2 in their B cells and developed significantly increased percentages and numbers of B cells and plasma cells, serum levels of IgG autoantibodies, glomerular deposition of IgG and C3, and severity of glomerular and tubulointerstitial inflammation, culminating in severe proteinuria and death (all P < 0.05 versus NZM.Baff(-/-) littermates). The time course for development of SLE-like features in NZM.Baff(-/-) .Bcl2(Tg) mice was more rapid than has been previously observed in NZM 2328 wild-type mice (median age at death 4.5 months versus 7.5 months). NZM.Baff(-/-) .Bcl2(Tg) mice remained responsive to BAFF, since reintroduction of the Baff gene into these mice further accelerated the course of disease (median age at death 3 months). CONCLUSION: The role of BAFF in the development of SLE-like disease may be dispensable as long as B cell survival is preserved via a BAFF-independent pathway. This may help explain the limited and variable clinical success with BAFF antagonists in human SLE. Thus, NZM.Baff(-/-) .Bcl2(Tg) mice may serve as a powerful murine model for the study of BAFF-independent SLE.
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